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阿立哌唑对人体静脉注射可卡因及吸烟的自我给药行为和药效学的影响。

Aripiprazole effects on self-administration and pharmacodynamics of intravenous cocaine and cigarette smoking in humans.

作者信息

Lofwall Michelle R, Nuzzo Paul A, Campbell Charles, Walsh Sharon L

机构信息

Department of Behavioral Science, Center on Drug and Alcohol Research.

Department of Cardiology.

出版信息

Exp Clin Psychopharmacol. 2014 Jun;22(3):238-47. doi: 10.1037/a0035165. Epub 2014 Jan 27.

Abstract

Aripiprazole is a partial agonist at dopamine (D2) and serotonin (5-HT1a) receptors and 5-HT2 antagonist. Because cocaine affects dopamine and serotonin, this study assessed whether aripiprazole could diminish the reinforcing efficacy of cocaine. Secondary aims evaluated aripiprazole on ad lib cigarette smoking and with a novel 40-hr smoking abstinence procedure. Adults with regular cocaine and cigarette use completed this inpatient double blind, randomized, placebo-controlled mixed-design study. A placebo lead-in was followed by randomization to aripiprazole (0, 2 or 10 mg/day/p.o.; n = 7 completed/group). Three sets of test sessions, each consisting of 3 cocaine sample-choice (i.e., self-administration) sessions and 1 dose-response session, were conducted (once during the lead-in and twice after randomization). Sample sessions tested each cocaine dose (0, 20 and 40 mg/70 kg, i.v.) in random order; subjective, observer-rated and physiologic outcomes were collected. Later that day, participants chose between the morning's sample dose or descending amounts of money over 7 trials. In dose response sessions, all doses were given 1 hr apart in ascending order for pharmacodynamic and pharmacokinetic assessment. Two sets of smoking topography sessions were conducted during the lead-in and after randomization; 1 with and 1 without 40 hr of smoking abstinence. Number of ad lib cigarettes smoked during non-session days was collected. Cocaine produced prototypic effects, but aripiprazole did not significantly alter these effects or smoking outcomes. The smoking abstinence procedure reliably produced nicotine withdrawal and craving and increased smoking modestly. These data do not support further investigation of aripiprazole for cocaine or tobacco use disorder treatment.

摘要

阿立哌唑是多巴胺(D2)和5-羟色胺(5-HT1a)受体的部分激动剂以及5-HT2拮抗剂。由于可卡因会影响多巴胺和5-羟色胺,本研究评估了阿立哌唑是否能降低可卡因的强化效力。次要目的是评估阿立哌唑对随意吸烟以及一种新的40小时戒烟程序的影响。有规律使用可卡因和香烟的成年人完成了这项住院双盲、随机、安慰剂对照的混合设计研究。在安慰剂导入期之后,随机分为阿立哌唑组(0、2或每日10毫克/口服;每组7人完成)。进行了三组测试环节,每组包括3次可卡因样本选择(即自我给药)环节和1次剂量反应环节(在导入期进行1次,随机分组后进行2次)。样本环节以随机顺序测试每种可卡因剂量(0、20和40毫克/70千克,静脉注射);收集主观、观察者评定和生理结果。当天晚些时候,参与者在上午的样本剂量或7次试验中逐渐减少的金钱数额之间进行选择。在剂量反应环节,所有剂量按升序每隔1小时给药一次,用于药效学和药代动力学评估。在导入期和随机分组后进行了两组吸烟行为记录环节;一组有40小时戒烟期,另一组没有。收集非测试日的随意吸烟数量。可卡因产生了典型效应,但阿立哌唑并未显著改变这些效应或吸烟结果。戒烟程序可靠地产生了尼古丁戒断和渴望,并适度增加了吸烟量。这些数据不支持进一步研究阿立哌唑用于治疗可卡因或烟草使用障碍。

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